PUBLICATION

Spinal Muscular Atrophy Associated with Progressive Myoclonic Epilepsy Is Caused by Mutations in ASAH1

Authors
Zhou, J., Tawk, M., Tiziano, F.D., Veillet, J., Bayes, M., Nolent, F., Garcia, V., Servidei, S., Bertini, E., Castro-Giner, F., Renda, Y., Carpentier, S., Andrieu-Abadie, N., Gut, I., Levade, T., Topaloglu, H., and Melki, J.
ID
ZDB-PUB-120702-10
Date
2012
Source
American journal of human genetics   91(1): 5-14 (Journal)
Registered Authors
Tawk, Marcel
Keywords
none
MeSH Terms
  • Acid Ceramidase/genetics*
  • Adolescent
  • Animals
  • Child
  • Child, Preschool
  • Female
  • Gene Knockdown Techniques
  • Humans
  • Male
  • Mutation*
  • Myoclonic Epilepsies, Progressive/genetics
  • Pedigree
  • Spinal Muscular Atrophies of Childhood/genetics*
  • Zebrafish
(all 14)
PubMed
22703880 Full text @ Am. J. Hum. Genet.
Abstract

Spinal muscular atrophy (SMA) is a clinically and genetically heterogeneous disease characterized by the degeneration of lower motor neurons. The most frequent form is linked to mutations in SMN1. Childhood SMA associated with progressive myoclonic epilepsy (SMA-PME) has been reported as a rare autosomal-recessive condition unlinked to mutations in SMN1. Through linkage analysis, homozygosity mapping, and exome sequencing in three unrelated SMA-PME-affected families, we identified a homozygous missense mutation (c.125C>T [p.Thr42Met]) in exon 2 of ASAH1 in the affected children of two families and the same mutation associated with a deletion of the whole gene in the third family. Expression studies of the c.125C>T mutant cDNA in Farber fibroblasts showed that acid-ceramidase activity was only 32% of that generated by normal cDNA. This reduced activity was able to normalize the ceramide level in Farber cells, raising the question of the pathogenic mechanism underlying the CNS involvement in deficient cells. Morpholino knockdown of the ASAH1 ortholog in zebrafish led to a marked loss of motor-neuron axonal branching, a loss that is associated with increased apoptosis in the spinal cord. Our results reveal a wide phenotypic spectrum associated with ASAH1 mutations. An acid-ceramidase activity below 10% results in Farber disease, an early-onset disease starting with subcutaneous lipogranulomata, joint pain, and hoarseness of the voice, whereas a higher residual activity might be responsible for SMA-PME, a later-onset phenotype restricted to the CNS and starting with lower-motor-neuron disease.

Genes / Markers
Marker Marker Type Name
asah1bGENEN-acylsphingosine amidohydrolase (acid ceramidase) 1b
1 - 1 of 1
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Figures
No images available
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Expression
Phenotype
Fish Conditions Stage Phenotype Figure
WT + MO1-asah1bstandard conditionsLong-pec
WT + MO1-asah1bstandard conditionsLong-pec
WT + MO1-asah1bstandard conditionsLong-pec
WT + MO1-asah1bstandard conditionsLong-pec
WT + MO1-asah1bstandard conditionsLong-pec
1 - 5 of 5
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Mutations / Transgenics
No data available
Human Disease / Model
No data available
Sequence Targeting Reagents
Target Reagent Reagent Type
asah1bMO1-asah1bMRPHLNO
1 - 1 of 1
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Fish
Fish
WT
WT + MO1-asah1b
1 - 2 of 2
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Antibodies
Orthology
No data available
Engineered Foreign Genes
No data available
Mapping
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Citation
Zhou, J., Tawk, M., Tiziano, F.D., Veillet, J., Bayes, M., Nolent, F., Garcia, V., Servidei, S., Bertini, E., Castro-Giner, F., Renda, Y., Carpentier, S., Andrieu-Abadie, N., Gut, I., Levade, T., Topaloglu, H., and Melki, J. (2012) Spinal Muscular Atrophy Associated with Progressive Myoclonic Epilepsy Is Caused by Mutations in ASAH1. American journal of human genetics. 91(1):5-14.